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首页> 外文期刊>Clinical immunology: The official journal of the Clinical Immunology Society >Human platelets can discriminate between various bacterial LPS isoforms via TLR4 signaling and differential cytokine secretion
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Human platelets can discriminate between various bacterial LPS isoforms via TLR4 signaling and differential cytokine secretion

机译:人类血小板可以通过TLR4信号和不同的细胞因子分泌来区分各种细菌LPS亚型

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Platelets are currently acknowledged as cells of innate immunity and inflammation and play a complex role in sepsis. We examined whether different types of LPS have different effects on the release of soluble signaling/effective molecules from platelets. We used platelet-rich plasma from healthy volunteers and LPS from two strains of gram-negative bacteria with disparate LPS structures. We combined LPS-stimulated platelet supernatants with reporter cells and measured the PBMC cytokine secretion profiles. Upon stimulation of platelets with both Escherichia coli O111 and Salmonella minnesota LPS, the platelet LPS::TLR4 interaction activated pathways to trigger the production of a large number of molecules. The different platelet supernatants caused differential PBMC secretion of IL-6, TNFα, and IL-8. Our data demonstrate that platelets have the capacity to sense external signals differentially through a single type of pathogen recognition receptor and adjust the innate immune response appropriately for pathogens exhibiting different types of 'danger' signals.
机译:血小板目前被认为是先天免疫和炎症细胞,并在败血症中起着复杂的作用。我们检查了不同类型的LPS是否对血小板释放的可溶性信号/有效分子具有不同的影响。我们使用了来自健康志愿者的富含血小板的血浆和来自具有不同LPS结构的两种革兰氏阴性细菌菌株的LPS。我们将LPS刺激的血小板上清液与报告细胞相结合,并测量了PBMC细胞因子分泌特征。在用大肠杆菌O111和明尼苏达沙门氏菌LPS刺激血小板后,血小板LPS :: TLR4相互作用激活了途径来触发大量分子的产生。不同的血小板上清液引起IL-6,TNFα和IL-8的PBMC分泌差异。我们的数据表明,血小板具有通过单一类型的病原体识别受体差异感测外部信号的能力,并能够针对表现出不同类型“危险”信号的病原体适当调整先天免疫应答。

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